Journal
SCIENCE
Volume 375, Issue 6578, Pages 283-+Publisher
AMER ASSOC ADVANCEMENT SCIENCE
DOI: 10.1126/science.abj7662
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Funding
- EMBO long term fellowship [ALTF 1295-2015, ALTF 139-2018]
- Washington Research Foundation Innovation Fellowship
- Human Frontiers Science Program long term fellowship
- DARPA Biostasis [HR001118S0034]
- Open Philanthropy Project Improving Protein Design Fund
- Audacious Project at the Institute for Protein Design
- Howard Hughes Medical Research Institute
- NIH Resource for Native Mass Spectrometry Guided Structural Biology [P41 GM128577]
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This study demonstrates the successful generation of stable, folded, and soluble designs using implicit negative design, which can undergo subunit exchange to enable reconfiguration of various complexes. The approach provides a general route to designing asymmetric reconfigurable protein systems.
Asymmetric multiprotein complexes that undergo subunit exchange play central roles in biology but present a challenge for design because the components must not only contain interfaces that enable reversible association but also be stable and well behaved in isolation. We use implicit negative design to generate p sheet-mediated heterodimers that can be assembled into a wide variety of complexes. The designs are stable, folded, and soluble in isolation and rapidly assemble upon mixing, and crystal structures are close to the computational models. We construct linearly arranged hetero-oligomers with up to six different components, branched hetero-oligomers, closed C4-symmetric two-component rings, and hetero-oligomers assembled on a cyclic homo-oligomeric central hub and demonstrate that such complexes can readily reconfigure through subunit exchange. Our approach provides a general route to designing asymmetric reconfigurable protein systems.
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